antibiotic courses and antibiotic conservation, getting
TRANSCRIPT
Antibiotic courses and antibiotic conservation, getting the balance right
Prof Martin LlewelynBrighton and Sussex Medical School
Brighton and Sussex University Hospitals NHS Trust
The King's Fund: Ideas that change health care6 October 2017
Antibiotic resistance and antibiotic use
• Antibiotic resistance - a global, urgent threat to human health• Antibiotic overuse in humans is a key driver of antibiotic resistance• Optimisation of antibiotic prescribing - Antibiotic stewardship - involves
• But• Antibiotic decisions are made in individual consultations
• They lack evidence to guide individual – level risk / benefit analyses
”a set of coordinated strategies to improve the use of antimicrobial medications with the goal to enhance patient health outcomes, reduce antibiotic resistance, and decrease unnecessary costs”
“…the long-term effects of antimicrobial selection, dosage, and duration of treatment on resistance development should be a part of every antimicrobial treatment decision”1
1. McGowan, JE Jr,; Gerding D. "Does antibiotic restriction prevent resistance?" New Horizon. 4 (3): 370–6.
A time-line of stewardship in the UK
“we will cut inappropriate prescribing in the UK by half by 2020…”
https://www.cdc.gov/features/antibioticuse/
How much could antibiotic use be cut?“By 2020, significant outcomes will include:Reduction of inappropriate antibiotic use
By 50% in outpatient settingsBy 20% in inpatient settings”
Antibiotic resistance and antibiotic use
• Antibiotic resistance - a global, urgent threat to human health• Antibiotic overuse in humans is a key driver of antibiotic resistance• Optimisation of antibiotic prescribing - Antibiotic stewardship - involves
• But• Antibiotic decisions are made in individual consultations
• Prescribers lack evidence to guide individual – level risk / benefit analyses
”a set of coordinated strategies to improve the use of antimicrobial medications with the goal to enhance patient health outcomes, reduce antibiotic resistance, and decrease unnecessary costs”
“…the long-term effects of antimicrobial selection, dosage, and duration of treatment on resistance development should be a part of every antimicrobial treatment decision”1
1. McGowan, JE Jr,; Gerding D. "Does antibiotic restriction prevent resistance?" New Horizon. 4 (3): 370–6.
There are only two ways doctors can reduce patient-exposure to antibiotics
A safe and effective strategy in primary care• Many patients understand antibiotics
don’t treat viruses• Risk of failing to treat serious infection is
low• Positively re-enforces patient
understanding that antibiotics aren’t always needed
• Option 1: Don’t Start
frugalnurse.com
There are only two ways to reduce antibiotic use
• Option 2: Stop sooner
Review and Revise of the decision• Is infection really the right diagnosis?• Is the patient getting better?• Is it time to cut-back or stop?• A daily risk – benefit judgement for
the individual patient
Stopping antibiotics is hard to doPr
escr
iptio
ns w
ith 7
2-hr
revi
ew (%
)
Prescriptions stopped (%)
https://fingertips.phe.org.uk/profile/amr-local-indicators
Median About right?
Why is it so hard to stop taking antibiotics?
• We’ve been taught since school to ‘complete the course to avoid antibiotic resistance’.
• Studies have never been done to show how long a course should be
• We have no way of measuring when to stop
Why is it so hard to stop taking antibiotics?
• We’ve been taught since school to ‘complete the course to avoid antibiotic resistance’.
• Studies have never been done to show how long a course should be
• We have no way of measuring when to stop
Where does ‘complete the course to avoid antibiotic resistance’ come from?
11
Mr. X. has a sore throat. He buys some penicillin and gives himself, not enough to kill the streptococci but enough to educate them to resist penicillin. He then infectshis wife. Mrs. X gets pneumonia and is treated with penicillin. As the streptococciare now resistant to penicillin the treatment fails. Mrs. X dies. Who is primarily responsible for Mrs. X’s death? Why Mr. X whose negligent use of penicillin changed the nature of the microbe. Moral: If you use penicillin, use enough.
Resistance in targets, resistance in bystanders
• Target selection – resistance selection in the organism you are targeting. Can happen with ‘professional pathogens’ like TB, gonorrhoea. But the answer is really drug dosing and combinations, not prolonged therapy.
• Bystander selection – resistance selection in all the commensal organisms exposed to the antibiotics – skin, gut, environment. Reservoirs of future resistant infections – where antibiotic exposure correlates well with risk of resistance.
Why is it so hard to stop taking antibiotics?
• We’ve been taught since school to ‘complete the course to avoid antibiotic resistance’.
• Studies have never been done to show how long a course should be
• We have no way of measuring when to stop
Studies have never been done to show how long a course should be.
Treatment with quinolone antibiotics – 5-7 days shown to be adequateTreatment with beta-lactams – no evidence –recommendation is 10-14 days
There is a lack of evidence that these durations are minimums – especially for
all patients
Evidence that shorter courses are as good for a few specific scenarios
• 520 children• Randomized to 5 or 10 days co-amoxiclav
treatment• Primary outcome – clinical failure• short course group
• more clinical failure• more symptoms > day 6
Clinical failure• 5 days 77/229 (33%) vs• 10 days 39/238 (16%)
So treatment of otitis media for 10 days means 66% of children will have 5 days
unnecessary co-amoxiclav
Is this really what we should do?Are trials telling us what we need to
know?
‘reduced-duration antimicrobial treatment resulted in less favorable outcomes than
standard-duration treatment’
Why is it so hard to stop taking antibiotics?
• We’ve been taught since school to ‘complete the course to avoid antibiotic resistance’.
• Studies have never been done to show how long a course should be
• We have no way of measuring when to stop
We have no way of knowing when to stop
• Clinical response e.g. ‘feeling better’?• May under estimate - e.g. infections with a deep focus• May over estimate – e.g. infections where symptoms lag
• Biomarkers such as procalcitonin (PCT) do exist• Slow to be evaluated• Slower to be adopted• Only in secondary care
• Lack of evidence as trial end-points
Indication-specific, poorly evidenced durations, backed up by ’complete the course to avoid resistance’ drives antibiotic over use
In summary
• We need to make ‘stopping’ work better in secondary care where it is our best hope to reduce antibiotic over use
• We need to begin thinking about how we tailor antibiotic durations better in primary care, to individual patients and how they respond to treatment
• Major scientific challenges• Linking exposure to resistance• Developing endpoints
• Major practical challenges• Particularly in primary care• In developing country healthcare systems• Around communication
A five year programme grant for applied research funded by NIHR
Optimise Review and Revise of antibiotic prescribing in hospitals
http://www.arkstudy.ox.ac.uk/